astrocyte activation

Equivalencies: 0 | Classes: 0 | Children: 0 | Explore

Entity

Name: astrocyte activation
Namespace: go
Namespace Version: 20180921
Namespace URL: https://raw.githubusercontent.com/pharmacome/terminology/b46b65c3da259b6e86026514dfececab7c22a11b/external/go-names.belns

Appears in Networks 3

Amyloid β oligomers (AβOs) in Alzheimer’s disease v1.0.0

Adenosine A1 receptor antagonist 64627 alleviates axonopathy caused by human Tau ΔK280 v1.0.0

Inﬂammasome Involvement in Alzheimer’s Disease v1.0.0

In-Edges 7

a(HBP:HBP00018) causesNoChange bp(GO:"astrocyte activation") View Subject | View Object

On the contrary, no relationship between total Aβ plaque burden and number of astrocytes or neurons was found (da Rocha-Souto et al. 2011). PubMed:29196815

Appears in Networks:

Amyloid β oligomers (AβOs) in Alzheimer’s disease v1.0.0

Annotations

MeSH: Extracellular Space
Cell Ontology (CL): neuron
Confidence: High

a(HBP:HBP00074) increases bp(GO:"astrocyte activation") View Subject | View Object

Furthermore, it was demonstrated that AβO may not only injure the neurites of brain neurons, but also activate microglia and astrocyte response (Sondag et al. 2009). PubMed:29196815

Appears in Networks:

Amyloid β oligomers (AβOs) in Alzheimer’s disease v1.0.0

Annotations

MeSH: Extracellular Space
Cell Ontology (CL): neuron
Confidence: High

a(HBP:HBP00074) positiveCorrelation bp(GO:"astrocyte activation") View Subject | View Object

In addition, the load of AβO deposits significantly correlated with fibrillar Aβ plaque deposition as well as with neuronal loss and numbers of astrocytes, although not with memory deficits. PubMed:29196815

Appears in Networks:

Amyloid β oligomers (AβOs) in Alzheimer’s disease v1.0.0

Annotations

MeSH: Extracellular Space
Cell Ontology (CL): neuron
Confidence: High

p(HBP:"Tau isoform F (441 aa)", var("p.Lys280del")) negativeCorrelation bp(GO:"astrocyte activation") View Subject | View Object

Surprisingly, expression of neuronal activity marker cFos, astrocytic activity marker Gfap, and oxidative stress marker Hmox1 were reduced in the proaggregant Tau transgenic slices, whereas antiaggregant Tau transgenic slices were not different from littermate controls (Fig. 4A) PubMed:27671637

Appears in Networks:

Adenosine A1 receptor antagonist 64627 alleviates axonopathy caused by human Tau ΔK280 v1.0.0

p(MGI:Gfap) biomarkerFor bp(GO:"astrocyte activation") View Subject | View Object

Appears in Networks:

Adenosine A1 receptor antagonist 64627 alleviates axonopathy caused by human Tau ΔK280 v1.0.0

p(HGNC:IL18) increases bp(GO:"astrocyte activation") View Subject | View Object

It is noteworthy that IL-1 beta and IL-18 can activate various cell types, par- ticularly astrocytes and microglia to induce additional cytokine release involving IL-1 beta , IL-6, and IL-18, and also nitric oxide (NO) synthase that can stimulate production of free radical NO, leading to the forma- tion of peroxynitrite that denatures DNA and impairs cellular energy pathways [48, 49]. PubMed:27314526